KR20190003805A - A pharmaceutical composition comprising an amine derivative or a pharmaceutically acceptable salt thereof and a stabilizer having a low melting point which inhibits cancer cell growth - Google Patents

Abstract

The present invention relates to a pharmaceutical composition comprising a thienopyrimidine compound, or a pharmaceutically acceptable salt thereof, or a hydrate of a pharmaceutically acceptable salt thereof, and at least one low-melting point stabilizer inhibiting the production of a softener, ≪ / RTI > and to pharmaceutical formulations comprising the same.

Description

A pharmaceutical composition comprising an amine derivative or a pharmaceutically acceptable salt thereof and a stabilizer having a low melting point which inhibits cancer cell growth

The present invention relates to a pharmaceutical composition comprising an amine derivative or a pharmaceutically acceptable salt thereof or a hydrate of a pharmaceutically acceptable salt thereof and a stabilizer having a low melting point which effectively inhibits cancer cell growth, ≪ / RTI >

Cells are involved in a variety of signaling pathways. Such signaling pathways are organically linked to each other, forming a complex mechanism and regulating cell proliferation, growth, and death (William G. Kaelin et al. , Nature Reviews Cancer , 2005, 5: 689-698). Thus, if the intracellular regulatory function is imbalanced due to genetic or environmental causes, signal transduction is abnormally amplified or destroyed and causes diseases such as tumors (Douglas Hanahan et al ., The Hallmarks of Cancer, 2000, 100: 57-70).

Protein tyrosine kinases play an important role in intercellular signal transduction (Irena Melnikova, et al ., Targeting protein kinases , 2004, 3: 993-994), and abnormal expression or mutations thereof are frequently observed in cancer cells have. Protein tyrosine kinases are enzymes that catalyze the transfer of phosphate groups from ATP to tyrosine on a protein substrate. Many growth factor receptor proteins undergo intracellular signal transduction by such tyrosine kinase activity. The interaction between growth factors and their receptors is essential for normal regulation of cell growth. However, when the receptor-mediated signaling regulates dysfunction due to receptor mutation or over-expression, tumor cells develop and eventually cause cancer.

Numerous growth factors and their receptors have been studied for their role as protein tyrosine kinases. Among these, studies on epithelial growth factor (EGF) and its receptor (EGFR) tyrosine kinase have been actively conducted (Nancy E. Hynes et al., Nature Reviews Cancer , 2005, 5: 341-354). The EGFR tyrosine kinase, which includes the receptor portion and the tyrosine kinase portion, is located through the cell membrane and thus serves to transfer extracellular signals into cells.

The purity of the active ingredient in medicine is an important factor in providing a safe and effective pharmaceutical formulation. Medicinal suppositories can cause a variety of side effects at the time of treatment. The problematic drug substance is a flexible substance or an active ingredient which is not completely removable and / or a flexible substance which is produced in the final pharmaceutical / pharmaceutical formulation manufacturing process; And storage degradation products produced in the final pharmaceutical formulation by various environmental factors such as temperature, humidity, and light.

It is an object of the present invention to provide a pharmaceutical composition having a low level of softness after the preparation of the final pharmaceutical formulation, wherein the pharmaceutical composition comprises an amine derivative or a pharmaceutically acceptable salt thereof or a pharmaceutical composition thereof for inhibiting the growth of cancer cells ≪ / RTI > acceptable hydrates of the salts.

It is another object of the present invention to provide a pharmaceutical formulation comprising and including the above pharmaceutical composition.

In order to achieve the above object, the present invention provides a pharmaceutical composition comprising a compound represented by the formula (I) represented by the formula (1) as a pharmaceutically active ingredient (API), N- (3- (2- Nor [3,2- d ] pyrimidin-4-yloxy) phenyl) acrylamide, or a pharmaceutically acceptable salt or a hydrate of a pharmaceutically acceptable salt thereof; And one or more low melting point stabilizers, and optionally one or more pharmaceutically acceptable excipients.

[Chemical Formula 1]

The present invention relates to the use of a compound of formula I, or a pharmaceutically acceptable salt thereof, or a hydrate of a pharmaceutically acceptable salt thereof, and one or more low melting point stabilizers to treat cancer, tumors, inflammatory diseases, autoimmune diseases or immunities - a pharmaceutical composition for the prevention and / or treatment of mediated diseases.

In order to achieve the above object, the present invention also provides a pharmaceutical formulation comprising and including the pharmaceutical composition.

The pharmaceutical composition of the present invention provides a lower level of the level of the pharmaceutically active ingredient produced during the formulation process. Pharmaceutical formulations prepared using and including the above pharmaceutical compositions can maintain quality even during long-term storage.

Fig. 1 shows the stability test results in comparison with the tablets of Comparative Examples 1 to 4 in which the total amount (by weight%) of the resulting flexible substances produced in the preparation of the tablets of Example 1 was not included as a low-melting stabilizer in polyethylene glycol.
Figure 2 shows the results of the stability test comparing the total amount (by weight) of the resulting soft materials produced in the preparation of the tablets of Examples 1 and 4 with tablets of Comparative Example 5 without the tablets.
Figure 3 shows the stability test results comparing the total amount of the resulting soft materials (based on% by weight) in the preparation of the tablets of Examples 1 and 5 to 8, which contain polyethylene glycol but have different hardness.
Figure 4 shows the stability test results comparing the total amount (by weight%) produced in the preparation of the tablets of Examples 1 to 3 with the tablets of Comparative Examples 1 and 10 having different levels of polyethylene glycol.
Fig. 5 shows the results of the stability test comparing the total amount (based on% by weight) of the resulting flexible substances produced in the preparation of the tablet of Example 1 with the tablets of Comparative Examples 9 to 13 in which the polyethylene glycol was replaced by another low melting point stabilizer.
6 shows the stability test results of the total amount (based on% by weight) of the resulting soft materials produced in the preparation of the tablets of Example 1 compared to the tablets of Comparative Examples 6 to 9 without the low-melting point stabilizer.
7 is an X-ray powder diffraction (XRPD) pattern of a solid form 1X (a dihydrocarbyl hydrate of the compound of Formula 1, preferably a monohydrate) upon irradiation with a Cu-K _? Light source.
FIG. 8 is a graph showing the effect of ¹³ C cross polarization / magic angle spinning (CP / MAS) total side suppression (TOSS) solid phase nuclear magnetic resonance (ssNMR) on solid type 1X (dihydrocarbyl hydrate, preferably monohydrate, ) ¹³ C cross polarization / magic angle spinning total suppression of sidebands solid state nuclear magnetic resonance ( ¹³ C CP / MAS TOSS ssNMR).

The invention will now be described with reference to exemplary embodiments.

Unless otherwise stated, all terms including technical and scientific terms used herein have the same meaning as commonly understood by one of ordinary skill in the art to which this invention belongs. Unless otherwise indicated, however, the following terms have the meanings given throughout this specification as described below:

As used herein, the term (s) of the present invention, unless otherwise indicated, shall be construed in an asymmetric manner to encompass the range of numbers recognized by ordinary skill in the art as equivalent to the recited numerical values Quot; In many cases, these terms may include numbers rounded to the nearest significant number. Specifically, the term " about " means about 5%, preferably 1% to 2% of a certain value or range (e.g., range of weight, weight%, etc.). For example, " about 10% by weight " means 9.5% to 10.5% by weight, preferably 9.8% to 10.2% by weight.

Although exemplary methods or materials are described herein, other similar or equivalent are also within the scope of the present invention. All publications, which are hereby incorporated by reference, are hereby incorporated by reference in their entirety.

The present inventors have studied to prepare a pharmaceutical composition having improved stability comprising an amine derivative or a pharmaceutically acceptable salt thereof or a hydrate of a pharmaceutically acceptable salt thereof, which inhibits the growth of cancer cells. The inventors have found that the use of low melting point stabilizers in pharmaceutical compositions induces the pharmaceutical dosage formulations containing the specified softening material to contain a lower level of certain softening materials.

One aspect of the present invention is a pharmaceutical composition comprising a compound represented by formula (I) or a pharmaceutically acceptable salt thereof or a hydrate of a pharmaceutically acceptable salt thereof as a pharmaceutically active ingredient; One or more low melting point stabilizers and, optionally, one or more pharmaceutically acceptable excipients.

Hereinafter, the features and the kinds of the components of the pharmaceutical composition of the present invention will be described in more detail.

(1) a pharmaceutically active ingredient

In the pharmaceutical composition of the present invention, a compound of the formula (I) or a pharmaceutically acceptable salt thereof or a hydrate of a pharmaceutically acceptable salt thereof may be used as a pharmaceutically active ingredient (API).

[Chemical Formula 1]

The compound of formula 1 according to the present invention can be prepared by various methods, for example, by the method described in WO 2011/162515.

In the present invention, pharmaceutically acceptable salts may be those commonly used in the related art. Salts with inorganic acids such as hydrochloric acid, sulfuric acid, sulfuric acid, nitric acid, phosphoric acid, perchloric acid, bromic acid and the like; There may be mentioned formic acid, acetic acid, acetic acid, propionic acid, oxalic acid, succinic acid, citric acid, citric acid, malonic acid, malonic acid, tartaric acid, gluconic acid, lactic acid, gentisic acid, fumaric acid, lactobionic acid, salicylic acid, phthalic acid, , Aspartic acid, glutamic acid, camsylic acid, besylic acid, or an organic acid such as acetylsalicylic acid (aspirin). The pharmaceutically acceptable salt may be in the form of a metal salt by reaction with an alkali metal such as calcium, sodium, magnesium, strontium or potassium. However, the present invention is not limited thereto.

In one embodiment of the present invention, the pharmaceutically active ingredient is the hydrochloride salt of the compound of formula (I).

In one embodiment, the hydrochloride salt of the compound of Formula 1 is amorphous.

In another embodiment, the hydrochloride salt of the compound of Formula 1 is in a crystalline form.

In one particular embodiment of the present invention, the crystalline hydrochloride is anhydrate.

In another specific embodiment of the present invention, the crystalline hydrochloride is a hydrate.

In another embodiment, the crystalline hydrochloride is a dihydrochloride salt.

In a further particular embodiment, the dihydrochloride salt is a hydrate, preferably a monohydrate.

In another embodiment, the crystalline hydrochloride is monohydrochloride.

In yet another embodiment, the monohydrochloride is a hydrate.

The crystalline form of the salt of the compound of formula

The salt of the compound of Formula 1 may be prepared in crystalline form, amorphous form, or a mixture thereof, preferably in a crystalline form. The crystalline form of the hydrochloride salt of the compound of formula (1), especially the crystalline form of the dihydrochloride monohydrate, is preferred in that it has excellent stability and therefore has physicochemical properties to facilitate formulation.

In one embodiment of the pharmaceutical composition of the present invention, the crystalline form of the dihydrohalide hydrate, preferably the dihydrochloride monohydrate, is a pharmaceutically active ingredient (API). Most preferably, the dihydrochloride monohydrate is a crystalline form designated 1X (see PCT / KR2016 / 015535). The crystalline form 1X has high water solubility, excellent non-hygroscopicity / non-wetting property and stability.

The preferred crystalline form 1X exhibits an X-ray powder diffraction (XRPD) pattern comprising peaks at diffraction angle 2 &thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG when irradiated with a Cu- .

More specifically, the crystalline form 1X shows an XRPD pattern comprising peaks at diffraction angle 2? Of 5.6 ° ± 0.2 °, 21.1 ° ± 0.2 °, and 27.3 ° ± 0.2 ° when irradiated with a Cu-Kα light source (XRPD1 -2).

More specifically, the crystalline form 1X shows an XRPD pattern including peaks at diffraction angle 2? Of 5.6 ° ± 0.2 °, 11.1 ° ± 0.2 °, and 27.3 ° ± 0.2 ° when irradiated with a Cu-Kα light source (XRPD1 -3).

More specifically, the crystalline form 1X contains peaks at diffraction angle 2? Of 5.6 ° ± 0.2 °, 11.1 ° ± 0.2 °, 21.1 ° ± 0.2 °, and 27.3 ° ± 0.2 ° when irradiated with a Cu-Kα light source Represents the XRPD pattern (XRPD1-4).

More specifically, the crystalline form 1X contains peaks at diffraction angle 2? Of 5.6 ° ± 0.2 °, 11.1 ° ± 0.2 °, 14.0 ° ± 0.2 °, and 27.3 ° ± 0.2 ° when irradiated with a Cu-Kα light source Represents the XRPD pattern (XRPD1-5).

More specifically, the crystalline form 1X has a composition of 5.6 ° ± 0.2 °, 11.1 ° ± 0.2 °, 14.0 ° ± 0.2 °, 20.8 ° ± 0.2 °, 21.1 ° ± 0.2 °, and 27.3 ° ± Gt; XRPD < / RTI > pattern containing peaks at a diffraction angle 2 &thetas; of 0.2 DEG (XRPD1-6).

More specifically, the crystalline form 1X has a composition of 5.6 ° ± 0.2 °, 10.7 ° ± 0.2 °, 11.1 ° ± 0.2 °, 14.0 ° ± 0.2 °, 20.8 ° ± 0.2 °, and 21.1 ° ± 0.2 ° when irradiated with a Cu- °, 22.5 ° ± 0.2 °, and 27.3 ° ± 0.2 ° (XRPD1-7).

The peaks may have a relative intensity (I / Io) of at least about 10%.

More specifically, the crystalline form 1 X represents an XRPD pattern having peaks at the diffraction angles as contained in Table A when irradiated with a Cu-K? Light source.

[Table A]

More specifically, the crystalline form 1X has the characteristics of an XRPD pattern as shown in FIG. 7 when irradiated with a Cu-K? Light source.

The crystalline form 1X may contain peaks at ¹³ C chemical shifts of its ¹³ C CP / MAS TOSS ssNMR spectra of 44.6 ± 0.2 ppm and 56.6 ± 0.2 ppm (ssNMR1-1).

More specifically, the crystalline form 1X may include peaks in ¹³ C chemical shifts of its ¹³ C CP / MAS TOSS ssNMR spectra of 44.6 ± 0.2 ppm, 45.4 ± 0.2 ppm, 50.8 ± 0.2 ppm, and 56.6 ± 0.2 ppm (SsNMR1-2).

The crystalline form 1X may contain peaks in the ¹³ C chemical shifts of its ¹³ C CP / MAS TOSS ssNMR spectra at 149.6 ± 0.2 ppm, 152.6 ± 0.2 ppm, and 164.3 ± 0.2 ppm (ssNMR1-3).

More specifically, the crystalline 1X is the ¹³ C CP / MAS TOSS ssNMR spectrum is 116.5 ± 0.2 ppm, 130.7 ± 0.2 ppm, 146.8 ± 0.2 ppm, 149.6 ± 0.2 ppm, 13 of 152.6 ± 0.2 ppm, and 164.3 ± 0.2 ppm C chemical shifts (ssNMR1-4).

More specifically, the crystalline form 1X exhibited the ¹³ C CP / MAS TOSS ssNMR spectra at ¹³ C chemical shifts of 44.6 ± 0.2 ppm, 56.6 ± 0.2 ppm, 149.6 ± 0.2 ppm, 152.6 ± 0.2 ppm, and 164.3 ± 0.2 ppm Peaks (ssNMR1-5).

More specifically, the crystalline form 1X may contain peaks in the ¹³ C chemical shifts as indicated in the following Table B (representing ppm < RTI ID = 0.0 > + -0.2 ppm) < / RTI > in its ¹³ C CP / MAS TOSS ssNMR spectrum:

[Table B]

More specifically, the crystalline form 1X has the characteristics of the ¹³ C CP / MAS TOSS ssNMR spectrum shown in FIG. 8 when irradiated with a Cu-K? Light source.

The crystalline form 1X may have the following characteristics:

(a) an XRPD pattern comprising peaks at diffraction angle 2 &thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG when irradiated with a Cu-K? light source; And

(b) ¹³ C CP / MAS TOSS ssNMR containing peaks in ¹³ C chemical shifts of 44.6 + - 0.2 ppm and 56.6 + - 0.2 ppm.

The crystalline form 1X may have the following characteristics:

(a) an XRPD pattern comprising peaks at diffraction angle 2 &thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG when irradiated with a Cu-K? light source; And

(b) ¹³ C CP / MAS TOSS ssNMR containing peaks at ¹³ C chemical shifts of 149.6 ± 0.2 ppm, 152.6 ± 0.2 ppm, and 164.3 ± 0.2 ppm.

The crystalline form (e. G., 1) may also be characterized by any other combination of XRPD peaks (XRPD1-1 to XRPD1-7) and 13C chemical shifts (ssNMR1-1 to ssNMR1-5) described above.

XRPD analysis of the samples was performed using a D8 Advance (Bruker ASX, Germany) analyzer in the range of 3 2? To 40 2 ?. If the amount of the sample is less than 100 mg, about 5 mg to 10 mg of the sample is gently squeezed onto the glass slide fixed to the sample holder. If the amount of the sample is more than 100 mg, about 100 mg of the sample is gently squeezed into the plastic sample holder so that the sample surface is smooth and placed just above the sample holder level.

The measurements were performed as follows:

Cathode material (K?): Cu K? (1.54056 A)

Scanning range: 3 ° to 40 °

Generator settings: 100 mA, 40.0 kV

Scanning speed: 1 sec / step

Diver slit: 0.3 °

Anti-scatter slit: 0.3 °

Temperature: 20 ° C

Step size: 0.02 ° 2θ

Rotation: Use

Goniometer Radius: 435 mm.

Solid State Nuclear Magnetic Resonance Spectroscopy (SSNMR) was performed on a solid phase, for example, as follows.

A 100 mg sample was weighed and added to a 4 mm sample tube. ^{The 13} C NMR spectrum ( ¹³ C CP / MAS TOSS ssNMR) was run on a Bruker Avance II 500 MHz Solid NMR system (Bruker, Germany) analyzer with a 4 mm probe type CP / MAS BB- Lt; RTI ID = 0.0 >

Frequency: 125.76 MHz,

Spectrum width: 20 kHz,

Rotation speed of sample at magic angle: 5 kHz,

Pulse sequence: Cross Polarization (CP) with decoupling SPINAL64 (80 kHz decoupling power)

Delay repeats: 5 seconds

Contact time: 2 ms

Number of Scans: 4096.

External standard: adamantane

The crystalline form 1X can have a water content of about 3.1% (measured by a Karl Fischer titrator (795 KFT Titrino, Metrohm, Switzerland) (theoretical moisture content of monohydrate is 3.11%), differential scanning calorimetry STA-1000, Scinco, Korea), the melting point may be about 202 占 폚 to 225 占 폚.

In one embodiment, the pharmaceutical composition according to the present invention comprises the hydrochloride salt of the compound of formula 1 as a pharmaceutically active ingredient, wherein at least 50% by weight of the pharmaceutically active ingredient is present in a crystalline form 1X as described above do. Preferably, at least 80%, more preferably at least 90%, most preferably at least 95% by weight of the pharmaceutically active ingredient in the pharmaceutical composition is present in crystalline form 1X as defined above do.

The pharmacologically active ingredient is contained in an effective weight to exhibit pharmacological activity, and may be in the form of a compound of Formula 1 in an amount of from 1 mg to 1,000 mg, for example, 50 mg or 75 mg per unit dosage form of the present invention Or 150 mg or 200 mg or 400 mg or 600 mg or 800 mg, or a pharmaceutically acceptable salt, or a pharmaceutically acceptable salt, or hydrate of a corresponding weight thereof. In one embodiment, the amount of monohydrate monohydrate per unit pharmaceutical formulation is an amount corresponding to 200 mg of the free base (Formula I). In another embodiment, the amount of the monohydrate salt monohydrate per unit pharmaceutical formulation is an amount corresponding to 400 mg of the free base (Formula 1). The amount of the pharmaceutically active ingredient in the pharmaceutical composition is in the range of about 1% to 65%, preferably about 55% to 65% (by weight).

(2) Low melting point stabilizer

The pharmaceutical compositions of the present invention comprise one or more low melting point stabilizers having specific properties.

The low melting point stabilizers suitable for use in the pharmaceutical compositions according to the present invention inhibit the formation of certain flexible substances in the process of manufacturing formulations and have a melting point below 80 ° C. For example, the low melting point stabilizers may be selected from polyethylene glycols (e.g., PEG 1000, 1500, 1540, 2000, 3000, 4000, 6000, 8000, 20000 and 35000), glyceryl behenate, glyceryl monostearate, Sorbitan fatty acid esters such as sorbitan monopalmitate or sorbitan monostearate, polyoxyethylene-polyoxypropylene block copolymers such as polyoxyl 150 distearate and poloxamers such as poloxamers (e.g., 188 and 407), ethylene glycol Stearate, fatty acids having a melting point of 80 캜 or lower such as lauric acid, palmitic acid or stearic acid, and any mixture thereof.

The low melting point stabilizer may be about 0.15 to 0.6 part by weight based on 1 part by weight of the pharmaceutically active ingredient. The low melting point stabilizers used in this range provide a reduction in the production of the soft materials without compromising processability and drug release properties, for example, in the preparation of formulations, for example in the production of tablets.

In one embodiment of the pharmaceutical composition of the present invention, the low melting point stabilizer is polyethylene glycol. In one embodiment, polyethylene glycol having a molecular weight of from 1,000 to 35,000 is used. In another embodiment, polyethylene glycol having a molecular weight of from 1,000 to 8,000 is used. For example, a molecular weight range of 2,000 to 8,000 can be preferably used in solid formulations. Properties such as melting point may vary depending on the grade. For example, PEG 8000, also referred to as Macrogol 8000 (Ph. Eur.), Is most preferred and has a low melting point of 55 ° C to 63 ° C

In another embodiment, the low melting point stabilizer is present in an amount of from about 0.15 parts by weight to about 0.6 parts by weight, more specifically from about 0.2 parts by weight to 0.5 parts by weight, more specifically from about 0.2 parts by weight to 0.3% by weight, And still more specifically about 0.21 part by weight to 0.26 part by weight of polyethylene glycol. Preferably, the polyethylene glycol used is PEG 8000.

While not intending to limit the working principles of the present invention by a particular theory, it is believed that the low melting point stabilizer provides protection against friction, merely in order to better understand the present invention:

Upon dry granulation and compression, pressure is applied to the pharmaceutical composition. Particles in the powder mixture migrate, and the mixture becomes denser. The particle motion causes friction between the particles and may be responsible for an increase in certain softening agents in the core tablet formulation. Low melting point stabilizers such as polyethylene glycol 8000 (PEG 8000) can act as stabilizers because they protect the pharmaceutically active ingredient from mechanical stresses during dry granulation and compression.

When the low melting point stabilizer is used in an amount of less than about 0.15 part by weight, the formation of the flexible material may not be inhibited. When the low melting point stabilizer is used in an amount of about 0.6 parts by weight or more, problems may occur in drug release.

(3) a pharmaceutically acceptable excipient

The pharmaceutical compositions according to the present invention may comprise one or more pharmaceutically acceptable excipients. Such pharmaceutically acceptable excipients may be those commonly used in the art. For example, the pharmaceutically acceptable excipient may be selected from the group consisting of diluents, binders, disintegrants, lubricants, colorants, fluidizers, adsorbents, and any mixtures thereof, and any excipients commonly used in the pharmaceutical arts Lt; / RTI >

Diluents (also referred to as fillers) can increase the size of solid pharmaceutical compositions to produce pharmaceutical formulations containing pharmaceutical compositions that are easier for patients and caregivers to handle. Diluents used in pharmaceutical compositions include diluents commonly used in solid pharmaceutical compositions. In one embodiment of the invention, the diluent is: a solid organic material,

- sugars

(Such as monosaccharides such as glucose, oligosaccharides such as sucrose, or various crystalline modifications of lactose treated with disaccharides, precipitated, spray dried, drum dried or with additional excipients such as microcrystalline cellulose, or sorbitol, mannitol, Xylitol, lactitol, erythritol, dulcitol, ribitol, erythritol);

Celluloses and derivatives thereof (e.g., powdered cellulose or microcrystalline cellulose);

Starch or modified starch (e.g., pregelatinized starch, or partially hydrolyzed starch);

Or as a solid inorganic material,

- calcium phosphate, dibasic calcium phosphate, hydroxyapatite, calcium sulfate, calcium carbonate;

Or semi-

- lipid or paraffin;

And mixtures thereof, but is not limited thereto. Preferred diluents are mannitol and microcrystalline cellulose or mixtures thereof.

The diluent may be included in an amount of about 2 to 50 wt%, specifically about 5 to 40 wt%, more specifically about 8 to 30 wt%, and preferably about 10 to 25 wt%, based on the total weight of the pharmaceutical composition .

Binders help bind the pharmaceutically active ingredient and other excipients together. Binders that may be used in pharmaceutical compositions include binders that are commonly used in solid pharmaceutical compositions. In one embodiment of the present invention, the binder may be selected from the group consisting of but not limited thereto. A preferred binding agent is hydroxypropylcellulose:

- cellulose and / or derivatives thereof such as ethylcellulose, carboxymethylcellulose, hydroxypropylmethylcellulose, hydroxypropylcellulose, hydroxyethylcellulose;

- starches or modified starches (e.g., pregelatinized starches or partially hydrolyzed starches);

- polyvinylpyrrolidone (e.g. Kollidon K30), polyvinyl acetate, polyvinyl alcohol or copolymers thereof such as Copovidone;

And mixtures thereof. However, the present invention is not limited thereto. Preferably the binder is hydroxypropylcellulose.

The binder may be included in an amount of from about 1 to 25% by weight, specifically about 1 to 10% by weight, more specifically about 1 to 5% by weight, and preferably about 3% by weight, based on the total weight of the pharmaceutical composition.

Disintegration increases the solubility of the solid pharmaceutical composition in the body of a patient. Disintegrants used in such pharmaceutical compositions include disintegrants commonly used in solid pharmaceutical compositions. In one embodiment of the invention, the disintegrant is selected from the group consisting of, but not limited to, sodium starch glycolate, crospovidone, croscarmellose, sodium carboxymethylcellulose, and dried corn starch, and any mixtures thereof. A preferred disintegrant is crospovidone.

The disintegrant may be contained in an amount of about 1 to 30% by weight, specifically about 2 to 6% by weight, and preferably about 3% by weight, based on the total weight of the pharmaceutical composition.

The lubricant is added to the pharmaceutical composition to facilitate the process by preventing sticking to the equipment during processing. Glidants used in pharmaceutical compositions include glidants commonly used in solid pharmaceutical compositions. In one embodiment of the invention, the lubricant is selected from the group consisting of stearic acid, magnesium stearate, calcium stearate, sodium stearyl fumarate, glycerol tribehenate, polyethylene glycol, and any mixture thereof, It is not. A preferred lubricant is magnesium stearate.

The lubricant may be contained in an amount of about 0.5 to 5% by weight, specifically 0.5 to 2% by weight, and preferably about 1% by weight, based on the total weight of the pharmaceutical composition.

The fluidizing agent improves the flowability of the uncompressed solid pharmaceutical composition and improves the administration accuracy. The fluidizing agent used in the pharmaceutical composition comprises a fluidizing agent generally used in solid pharmaceutical compositions. The fluidizing agents that may be used in the pharmaceutical compositions include, but are not limited to, colloidal silicon dioxide, magnesium trisilicate, starch, talc, calcium phosphate, and any combination thereof.

If there is ambiguity in naming the stabilizers or any of the excipients described herein (ie, due to differences in the pharmacopoeia depending on the area), it follows the European Pharmacopoeia.

Accordingly, in one aspect, the invention provides pharmaceutical dosage forms prepared using and including the pharmaceutical compositions as described above.

In one embodiment, the pharmaceutical formulation is a solid dosage form. In another embodiment, the pharmaceutical formulation is a liquid formulation. For example, the pharmaceutical formulation is a syrup. In one embodiment, the pharmaceutical formulation is a tablet. Such tablets may be formulated by compression and tabletting methods well known in the art, and may be formulated by dry granulation or wet granulation using, for example, processing aids such as solvents.

As an example of a pharmaceutical formulation according to the present invention, tablets may have a hardness between 6 kp and 22 kp. When the tablet of the present invention has a hardness of less than 6 kp, the friability can be increased, and when the hardness of the tablet of the present invention is more than 22 kp, the dissolution rate can be reduced.

In order to prevent contact with the user's hands or skin when dealing with the solid pharmaceutical dosage form according to the invention, the pharmaceutical composition may comprise a coating, that is to say a release film forming agent, an enteric coating agent, Coatings, and any mixture thereof. In one more specific embodiment of the pharmaceutical compositions and the pharmaceutical formulations, such coatings may additionally include colorants / pigments such as iron oxide or titanium dioxide, or plasticizers.

Exemplary coatings used in the present invention include hydroxypropylcellulose, hydroxypropylmethylcellulose, polyvinylalcohol and polyvinyl alcohol-polyethylene glycol graft polymer (Kollicoat IR, BASF) as immediate release film former; As an enteric coating agent, a (meth) acrylic acid copolymer (EUDRAGIT, Evonik Industries), hydroxypropylmethylcellulose phthalate, and phthalic acid cellulose acetate; And cellulose acetate, ethylcellulose, and polyvinyl acetate as sustained-release coatings.

The coating agent may be contained in an amount of 1 to 10% by weight, preferably 1 to 5% by weight, more preferably 2 to 4% by weight, based on the total weight of the pharmaceutical composition before coating.

Yet another embodiment of the pharmaceutical composition according to the present invention is as follows:

General description of refining core manufacturing process:

Step 1.1 (I. E., A compound of formula (I) of any of the forms described herein, preferably a dihydrochloride monohydrate), a portion of magnesium stearate, hydroxypropylcellulose, microcrystalline cellulose and Mannitol is mixed.

Step 1.2 Dry granulation: The pre-mix of the pre-mixing step 1.1 is dry granulated using a dry granulator to obtain granules.

Step 2 Mixing: Crospovidone and residual magnesium stearate are added to the granules obtained in step 1.2 in one step or a subsequent step to obtain a final blend.

Step 3 Tablet core: The final blend from the previous step is compressed into a tablet core using a tablet machine.

General description of the process for the preparation of film-coated tablets (starting from the tablet cores obtained in steps 1 to 3):

Step 4.1 Dispersion: A ready-to-use coating mixture is suspended in a mixture of purified water and alcohol at room temperature to obtain a film-coated suspension.

Step 4.2 Film coating: The tabular core obtained in step 3 is coated with the film coating suspension of step 4.1.

The pharmaceutical composition of the present invention and the pharmaceutical formulation prepared using the same include a compound of Formula 1 (or a salt, a hydrate, a salt thereof as described above), and the epithelial growth factor receptor tyrosine kinase or a mutant thereof Lt; RTI ID = 0.0 > tumor < / RTI >

The pharmaceutical compositions of the present invention and the pharmaceutical formulations comprising and using them can be used for the prevention and / or treatment of cancer, tumors, inflammatory diseases, autoimmune diseases or immune-mediated diseases.

The cancer or tumor may be a cancer cell or tumor caused by an epithelial cell growth factor receptor tyrosine kinase or a variant thereof wherein the variant is a wild type EGFR kinase sequence due to one or more mutations such as substitution, Lt; RTI ID = 0.0 > EGFR < / RTI > kinase. The EGFR tyrosine kinase-induced cancer or tumor can be, for example, liver cancer, hepatocellular carcinoma, thyroid cancer, colon cancer, testicular cancer, osteocarcinoma, basal cell carcinoma, ovarian cancer, brain tumor, gallbladder carcinoma, head and neck cancer, , Cancer of the bladder, stomach cancer, esophageal cancer, glioma, glioblastoma, renal cancer, malignant tumor, gastric cancer, breast cancer, sarcoma, parietal cancer, uterine cancer, cervical cancer, prostate cancer, rectal cancer, pancreatic cancer, lung cancer, skin cancer, But is not limited thereto.

In one embodiment, the EGFR tyrosine kinase-inducing cancer is lung cancer. In one embodiment, the lung cancer is selected from non-small cell lung cancer (NSCLC, e.g. locally advanced or metastatic NSCLC (IIIB / IV), NSCLC abortion cancer, flat tissue NSCLC, , Especially NSCLC abortion cancer.

In one embodiment, the EGFR tyrosine kinase-inducing cancer involves EGFR exon 20 insertion or EGFR exon 19 deletion (Del19) or EGFR L858R mutation or EGFR T790M mutation, or any combination thereof.

In one embodiment, the EGFR tyrosine kinase-induced cancer comprises at least one EGFR mutation, wherein the mutation is selected from one or more EGFR mutations in Del19 (exon 19 deletion), L858R and T790M, and any combination thereof.

In one embodiment, the EGFR tyrosine kinase-induced cancer is accompanied by an EGFR mutation Del19.

In one embodiment, the EGFR tyrosine kinase-induced cancer is accompanied by an EGFR L858R mutation.

In one embodiment, the EGFR tyrosine kinase-induced cancer is accompanied by an EGFR T790M mutation.

In one embodiment, the EGFR tyrosine kinase-induced cancer involves at least two EGFR mutations selected from the group consisting of Del19 / T790M and L858R / T790M.

In one embodiment, the EGFR tyrosine kinase-inducing cancer is a non-small cell lung cancer (NSCLC), particularly an NSCLC lung cancer, that is EGFR exon 20 insertion or EGFR exon 19 deletion (Del19) or EGFR L858R mutation or EGFR T790M mutation, Accompanied by a combination.

In one embodiment, the EGFR tyrosine kinase-inducing cancer is non-small cell lung cancer (NSCLC), particularly NSCLC lung cancer, with at least one EGFR mutation, wherein at least one EGFR mutation is Del19 (exon 19 deletion), L858R and T790M, And any combination thereof.

In one embodiment, the EGFR tyrosine kinase-inducing cancer is non-small cell lung cancer (NSCLC), particularly NSCLC lung cancer, involving at least two EGFR mutations selected from the group consisting of Del19 / T790M and L858R / T790M.

In one embodiment, the EGFR tyrosine kinase-inducing cancer is accompanied by an EGFR mutation Del199 in non-small cell lung cancer (NSCLC), particularly NSCLC lung cancer.

In one embodiment, the EGFR tyrosine kinase-induced cancer is accompanied by an EGFR mutation L858R in non-small cell lung cancer (NSCLC), particularly NSCLC lung cancer.

In one embodiment, the EGFR tyrosine kinase-induced cancer is accompanied by an EGFR mutation T790M in non-small cell lung cancer (NSCLC), particularly NSCLC lung cancer.

For example, inflammatory diseases, autoimmune diseases or immune-mediated diseases may be associated with arthritis, rheumatoid arthritis, spondyloarthropathies, gouty arthritis, osteoarthritis, juvenile arthritis, other arthritic conditions, lupus, systemic lupus erythematosus (SLE) (ARDS), pulmonary sarcoidosis, chronic pulmonary inflammatory disease, chronic obstructive pulmonary disease (COPD), cardiovascular disease, atherosclerosis, atherosclerosis, atherosclerosis, Inflammatory bowel disease, Crohn's disease, ulcerative colitis, irritable bowel syndrome, asthma, Sjogren's syndrome, autoimmune thyroid disease, urticaria, multiple sclerosis, scleroderma, organ transplant rejection , Xenotransplantation, chronic idiopathic thrombocytopenic purpura (ITP), Parkinson's disease, Alzheimer's disease, diabetes related disease, inflammation, pelvic inflammatory disease, allergic rhinitis, allergic (ALL), chronic lymphocytic leukemia (CLL), acute myelogenous leukemia (AML), chronic myelogenous leukemia (CML), leukemia, leukemia, lymphoma, B-cell lymphoma, T-cell lymphoma, myeloma CML), hairy cell leukemia, Hodgkin's lymphoma, multiple myeloma, myelodysplastic syndrome (MDS), myelodysplastic syndrome (MPN), diffuse large B cell lymphoma, and follicular lymphoma , But is not limited thereto.

Therefore, the present invention provides pharmaceutical compositions and pharmaceutical formulations as described herein for the prevention and / or treatment of cancer, tumors, inflammatory diseases, autoimmune diseases or immune-mediated diseases described herein.

The present invention also provides a method for preventing and / or treating cancer, tumor, inflammatory disease, autoimmune disease or immuno-mediated disease in a subject in need thereof. The method comprises administering a pharmaceutical composition or pharmaceutical dosage form of the invention in a subject in need thereof. The subject is, for example, a mammal, more particularly a human.

The pharmaceutical composition of the present invention may be administered through a number of routes such as oral, transdermal, subcutaneous, intravenous or intramuscular injection. The pharmaceutical composition of the present invention can be administered once or multiple times in a generally effective effective amount. However, the actual dosage of the pharmacologically active ingredient should be determined according to a number of related factors such as route of administration, age, sex and weight of the patient, and severity of the disease. Therefore, the dose does not limit the scope of the present invention in any respect.

The pharmaceutical composition of the present invention can be formulated into a conventional formulation in the field of pharmacy and can be administered orally, oromucosally, sublingually, rectally, intravaginally, topically or parenterally . Oral administration is preferred. For example, the pharmaceutical composition according to the present invention may be provided and (orally) administered in the form of a pharmaceutical dosage form. The pharmaceutical dosage form may be, for example, a tablet form containing starch or lactose, a capsule form which may contain excipients, or an elixir or syrup containing a flavoring or coloring agent, which may be administered orally, , ≪ / RTI > or sublingually. In addition, the pharmaceutical composition may be administered, for example, intravenously, intracavernosally, intramuscularly, subcutaneously and intravenously.

Hereinafter, the present invention will be described in detail by the following examples. However, the following examples are only illustrative of the present invention, and the scope of the present invention is not limited thereto.

Examples 1-3: Preparation of Tablets Containing Polyethylene Glycol

As the pharmaceutically active ingredient (API), the hydrochloride salt of the compound of formula (I) (Hanmi Fine Chemical Co.) was used. The API, mannitol (ROQUETTE), microcrystalline cellulose (MINGTAI), hydroxypropylcellulose (L-form, NISSO), and polyethylene glycol 8000 (Ph.Eur, Japan: Macrogol 6000, SANYO) The mixture was mixed according to the pharmaceutical composition, and the resulting mixture was dried and granulated using a roll compactor (TFC-LAB, FREUND).

Crospovidone (BASF) was added to and mixed with the granules prepared above, and magnesium stearate (PETER GREVEN) was added thereto to obtain the final mixture. Tablets with a hardness of 14 kp were prepared from the resulting mixture using a tablet machine (GRC-18, Sejong Pharmatech Co., Ltd.). The prepared tablets were coated with 2% by weight of Opadry Y-1-7000 (COLORCON) coating on the basis of the total weight of the tablets using an automatic coater (SFC-30, Sejong Pharmatech).

Example 1 Example 2 Example 3 Dry granule API 475 475 475 Mannitol 65 65 65 Microcrystalline cellulose 40 40 40 Hydroxypropylcellulose 20 20 20 Polyethylene glycol 8000 (Ph. Eur) (API basis weight part) 120 (0.25) 106 (0.22) 240 (0.51) mix Crospovidone 20 20 20 Final mixing Magnesium stearate 10 10 10 Gross weight (mg) 750 736 870 Purification hardness (kp) 14 14 14

Examples 4 to 8: Preparation of Tablets Containing Polyethylene Glycol

Tablets with the same pharmaceutical composition as in Example 1 shown in Table 2 were prepared, except that the hardness of the tablet was adjusted to 7 kp, 9 kp, 11 kp, or 18 kp. Example 4 was prepared without final tableting after final mixing.

Example 4 Example 5 Example 6 Example 7 Example 8 Dry granule API 475 475 475 475 475 Mannitol 65 65 65 65 65 Microcrystalline cellulose 40 40 40 40 40 cellulose Hydroxypropylcellulose 20 20 20 20 20 Polyethylene glycol 8000 (API basis weight part) 120 (0.25) 120 (0.25) 120 (0.25) 120 (0.25) 120 (0.25) mix Crospovidone 20 20 20 20 20 Final mixing Magnesium stearate 10 10 10 10 10 Gross weight (mg) 750 750 750 750 750 Purification hardness (kp) 0 7 9 11 18

Examples 9 to 18: Preparation of Tablets Containing Low Melting Point Stabilizers Other Than Polyethylene Glycol

Sorbitan monostearate, sorbitan monostearate, poloxamer 188, poloxamer 407, ethylene glycol stearate, glyceryl behenate, glyceryl monostearate, lauric acid, palmitic acid, or stearic acid with polyethylene glycol 8000 (Ph. Eur).

Example 9 Example 10 Example 11 Example 12 Example 13 Dry granule API 475 475 475 475 475 Mannitol 65 65 65 65 65 Microcrystalline cellulose 40 40 40 40 40 Hydroxypropylcellulose 20 20 20 20 20 Sorbitan 120 - - - - Monopalmitate Sorbitan monostearate - 120 - - - Poloxamer 188 - - 120 - - Poloxamer 407 - - - 120 - Ethylene glycol stearate - - - - 120 mix Crospovidone 20 20 20 20 20 Final mixing Magnesium stearate 10 10 10 10 10 Gross weight (mg) 750 750 750 750 750 Purification hardness (kp) 14 14 14 14 14

Example 14 Example 15 Example 16 Example 17 Example 18 Dry granule API 475 475 475 475 475 Mannitol 65 65 65 65 65 Microcrystalline cellulose 40 40 40 40 40 Hydroxypropylcellulose 20 20 20 20 20 Glyceryl behenate 120 - - - - Glyceryl monostearate - 120 - - - Lauric acid - - 120 - - Palmitic acid - - - 120 - Stearic acid - - - - 120 mix Crospovidone 20 20 20 20 20 Final mixing Magnesium stearate 10 10 10 10 10 Gross weight (mg) 750 750 750 750 750 Purification hardness (kp) 14 14 14 14 14

Comparative Examples 1 to 5: Preparation of tablets not containing polyethylene glycol

The tablets of Comparative Examples 1 to 4 were prepared with a hardness numerical value range of 9 to 18 kp in the same manner as in Example 1, except that no polyethylene glycol was added. Comparative Example 5 was produced after the final mixing without tableting process.

Comparative Example 1 Comparative Example 2 Comparative Example 3 Comparative Example 4 Comparative Example 5 Dry granule API 475 475 475 475 475 Mannitol 65 65 65 65 65 Microcrystalline cellulose 40 40 40 40 40 Hydroxypropylcellulose 20 20 20 20 20 mix Crospovidone 20 20 20 20 20 Final mixing Magnesium stearate 10 10 10 10 10 Gross weight (mg) 630 630 630 630 630 Purification hardness (kp) 14 9 11 18 0

Comparative Examples 6 to 10: Preparation of Tablets Containing Non-Low Melting Point Stabilizers

(Citric acid), ascorbic acid, magnesium carbonate, or magnesium oxide was used in place of polyethylene glycol 8000 (Ph. Eur.) In accordance with the composition shown in Table 7 below Tablets were prepared.

Comparative Example 6 Comparative Example 7 Comparative Example 8 Comparative Example 9 Comparative Example 10 Dry granule API 475 475 475 475 475 Mannitol 65 65 65 65 65 Microcrystalline cellulose 40 40 40 40 40 Hydroxypropylcellulose 20 20 20 20 20 Polyethylene glycol 8000 (Ph. Eur) - - - - 60 (0.13 parts by weight) Citric acid 120 - - - - Ascorbic acid - 120 - - - Magnesium carbonate - - 120 - - Magnesium oxide - - - 120 - mix Crospovidone 20 20 20 20 20 Final mixing Magnesium stearate 10 10 10 10 10 Gross weight (mg) 750 750 750 750 690 Purification hardness (kp) 14 14 14 14 14

Experimental Example 1: Determination of the content of a flexible substance

In order to evaluate the preparation of the preparations prepared in the above Examples and Comparative Examples, the total amount of the flexible substances was measured. The measurement and quantification of the flexible material were carried out as follows.

<Test Method>

Equipment used: High Performance Liquid Chromatography (HPLC, Hitachi 2000 series, Japan)

Detector: UV absorber (measuring wavelength: 254 nm)

Column: Inertsil ODS-2 (4.6 x 150 mm, 5 탆) or equivalent column

Flow rate: 1.0 mL / min

Column temperature: 30 DEG C

Mobile phase

<Calculation method>

The content of each softening material was determined by calculating the area under the corresponding peak in the chromatogram of high performance liquid chromatography (HPLC) under ultraviolet irradiation condition at 254 nm. The ratio of the peak area between the corresponding flux and the API was calculated in order to calculate all the flux content of all fluxes.

As shown in Tables 8 to 13 and Figs. 1 to 6, the pharmaceutical composition of the present invention containing the low melting point stabilizer can significantly inhibit all the flexible substances in the production of tablets. This improvement in manufacturing stability was more effective for certain flexible materials, such as those with relative retention time (RRT) of 1.4 or 1.8 in HPLC run according to the test method (data not shown).

Example 1 Comparative Example 1 Comparative Example 2 Comparative Example 3 Comparative Example 4 Total flexible material 0.615 0.733 0.702 0.718 0.735

As shown in Table 8 and FIG. 1, in the formulations of Comparative Examples 1 to 4 which did not contain a low-melting-point stabilizer, the total amount of initial softening substances immediately after preparation was compared with the formulation of Example 1 containing polyethylene glycol as a low- Respectively. In other words, in the comparative tablets tested after tabletting, more suppositories were observed and the hardness of the tablets increased.

To further examine the effect of stabilization at the time of manufacture, the following tablets (Example 1 and Comparative Example 1, both of Hardness 14) and non-tablet formulations (Example 5 and Comparative Example 5) were tested.

Example 1 Example 4 Comparative Example 1 Comparative Example 5 Total flexible material 0.615 0.402 0.733 0.497

As shown in Table 9 and Figure 2, this is consistent with the friction of the tableting stage which promotes the production of the softener while the tablet is being produced under increased pressure in the tablet machine.

Example 1 Example 5 Example 6 Example 7 Example 8 Total flexible material 0.615 0.627 0.610 0.611 0.621

As shown in Table 10 and Figure 3, when polyethylene glycol 8000 (Ph. Eur.) Was added to the formulation as a low melting point stabilizer, despite the difference in tablet hardness due to the difference in compressive force in the tabletting stage, , 5, 6, 7 and 8 showed that the level of total flexible material after manufacture was acceptable.

Comparative Example 1 Comparative Example 10 Example 2 Example 1 Example 3 Total flexible material 0.733 0.789 0.583 0.615 0.634

As shown in Table 11 and Figure 4, Comparative Example 1 had a high initial total flux after tableting. However, when it further contained 0.15 parts by weight or more of polyethylene glycol based on 1 part by weight of API, it provided significant inhibition of the softening to an acceptable level.

Example 1 Example 9 Example 10 Example 11 Example 12 Example 13 Total flexible material 0.615 0.610 0.612 0.620 0.625 0.632

The polyethylene glycol functions as a stabilizer and has a low melting point. Therefore, when the tablet is prepared by employing a low melting point stabilizer having properties similar to polyethylene glycol, as shown in Table 12 and Fig. 5, the stabilizer can be used to prevent friction even when the tablet is exposed to a high pressure in the tablet machine Thereby effectively inhibiting the production of a specific flexible substance from the API.

Example 1 Comparative Example 6 Comparative Example 7 Comparative Example 8 Comparative Example 9 Total flexible material 0.615 0.742 0.749 0.738 0.754

On the other hand, if tablets were prepared using stabilizers having a melting point of greater than 80 DEG C, the resulting formulations are similar to those of Comparative Example 1 where the flexible material profile is devoid of stabilizers, as shown in Table 13 and FIG. (3, 2-d] pyrimidin-4-yloxy) phenyl) acrylic acid as a pharmaceutically active ingredient, It can be concluded that the addition of a low melting stabilizer to the amide hydrochloride is important in ensuring a low level of flux after manufacture of the tablet.

Claims (43)

A pharmaceutical composition comprising:
As a pharmaceutically active ingredient, a compound represented by the formula (1) or a pharmaceutically acceptable salt thereof, or a hydrate of a pharmaceutically acceptable salt thereof
[Chemical Formula 1]

; And
One or more low melting point stabilizers having a melting point of 80 DEG C or less, and
Optionally, one or more pharmaceutically acceptable excipients. The pharmaceutical composition according to claim 1, wherein the pharmaceutically active ingredient is a hydrochloride salt of the compound of formula (1). The pharmaceutical composition according to claim 2, wherein the pharmaceutically active ingredient is a hydrochloride salt of the compound of formula (1). 4. The pharmaceutical composition according to claim 3, wherein the pharmaceutically active ingredient is a hydrate of the hydrochloride of the compound of formula (1). 4. The pharmaceutical composition according to claim 3, wherein the pharmaceutically active ingredient is a crystalline form of the dibasic acid salt of the compound of formula (1). The pharmaceutical composition according to claim 5, wherein the pharmaceutically active ingredient is a hydrate, preferably a monohydrate, of the compound of formula (I). The pharmaceutical composition according to claim 5, wherein the pharmacologically active ingredient has an X-ray powder diffraction (XRPD) pattern comprising peaks at diffraction angle 2 &amp;thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG when irradiated with a Cu- a pharmaceutical composition of the dihydrochloride crystal form of the compound of formula (I) containing a crystal form showing a 1X. 6. The pharmaceutical composition according to claim 5, wherein said pharmaceutically active ingredient is selected from the group consisting of crystalline 1X having the ¹³ C solid state NMR spectrum containing peaks in ¹³ C chemical shifts of 44.6 0.2 ppm and 56.6 0.2 ppm, Lt; / RTI &gt; is a crystalline form of dibasic acid. 6. The pharmaceutical composition according to claim 5, wherein the pharmaceutically active ingredient is crystalline 1X having a ¹³ C solid phase NMR spectrum comprising peaks at ¹³ C chemical shifts of 149.6 0.2 ppm, 152.6 0.2 ppm and 164.3 0.2 ppm. Lt; RTI ID = 0.0 &gt; (I) &lt; / RTI &gt; 6. The composition of claim 5, wherein the pharmaceutically active ingredient is
(a) an XRPD pattern comprising peaks at a diffraction angle 2 &amp;thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG when irradiated with a Cu-K? light source; And
(b) a crystal form 1X having a ¹³ C solid phase NMR spectrum comprising a peak at ¹³ C chemical shifts of 44.6 +/- 0.2 ppm and 56.6 +/- 0.2 ppm. 6. The composition of claim 5, wherein the pharmaceutically active ingredient is
(a) When irradiated with a Cu-K? light source. An XRPD pattern comprising peaks at diffraction angles 2 &amp;thetas; of 5.6 DEG +/- 0.2 DEG and 27.3 DEG +/- 0.2 DEG; And
(b) a crystalline form 1X having a ¹³ C solid phase NMR spectrum containing peaks at ¹³ C chemical shifts of 149.6 0.2 ppm, 152.6 0.2 ppm, and 164.3 0.2 ppm. &Lt; / RTI &gt; The pharmaceutical composition according to any one of claims 7 to 11, wherein at least 90 wt%, preferably at least 95 wt% of the pharmaceutically active ingredient is crystalline 1X. The pharmaceutical composition according to any one of the preceding claims, wherein said pharmaceutically active ingredient represents from about 1 to 65% by weight, based on the total weight of said composition. 7. The composition of any one of the preceding claims, wherein the one or more low melting point stabilizers having a melting point below 80 캜 are selected from the group consisting of polyethylene glycol, glyceryl behenate, glyceryl monostearate, sorbitan fatty acid ester, polyoxyethylene- Propylene block copolyol, and is selected from the group consisting of ethylene glycol stearate, fatty acids, and any mixture thereof. 15. The pharmaceutical composition according to claim 14, wherein the at least one low melting point stabilizer having a melting point of 80 DEG C or lower is polyethylene glycol, preferably polyethylene glycol having a molecular weight ranging from 1,000 to 8,000. The pharmaceutical composition according to claim 14, wherein the low melting point stabilizer having a melting point of 80 캜 or lower is PEG 8000. 15. The composition according to any one of claims 14 to 16, wherein the at least one low melting point stabilizer having a melting point of 80 캜 or less has a content of 0.15 to 0.6 parts by weight, relative to 1 part by weight of the pharmaceutically active ingredient, A pharmaceutical composition. The pharmaceutical composition according to any one of claims 1 to 17, wherein the pharmaceutical composition further comprises at least one diluent. 19. The pharmaceutical composition according to claim 18, wherein said at least one diluent is selected from mannitol, microcrystalline cellulose, and any mixture thereof. The pharmaceutical composition of any one of claims 18 and 19, wherein said at least one diluent represents from about 2 to 50 weight percent, based on the total weight of said composition. The pharmaceutical composition according to any one of claims 1 to 20, further comprising at least one binder. 22. The pharmaceutical composition according to claim 21, wherein the binder is hydroxypropylcellulose. 22. The pharmaceutical composition of claim 21 or 22, wherein said one or more binders represent about 1 to 25% by weight, based on the total weight of said composition. The pharmaceutical composition according to any one of claims 1 to 23, further comprising at least one disintegrant. 25. The pharmaceutical composition according to claim 24, wherein the disintegrant is crospovidone. 25. The pharmaceutical composition of claim 24 or 25, wherein said at least one disintegrant represents about 1 to 30% by weight, based on the total weight of said composition. The pharmaceutical composition of any one of claims 1 to 26, wherein said pharmaceutical composition further comprises at least one lubricant. 28. The pharmaceutical composition according to claim 27, wherein the lubricant is magnesium stearate. 29. The pharmaceutical composition of claim 27 or 28, wherein said at least one lubricant represents from about 0.5 to 5% by weight, based on the total weight of said composition. The pharmaceutical composition according to any one of claims 1 to 29, wherein the pharmaceutical composition further comprises at least one coating agent. 32. The pharmaceutical composition of claim 30, wherein the at least one coating agent represents from about 1 to 10% by weight, based on the total weight of the composition. The pharmaceutical composition according to claim 1, wherein the composition comprises:

The pharmaceutical composition according to claim 1, wherein the composition comprises:

A pharmaceutical formulation comprising a pharmaceutical composition according to any one of claims 1-33. 35. The pharmaceutical formulation of claim 34, wherein the formulation is a tablet. Comprising administering to a subject, preferably a person in need, a pharmaceutical composition according to any one of claims 1 to 33 or a pharmaceutical formulation according to claims 34 or 35, preferably in an individual A method of preventing and / or treating cancer, tumor, inflammatory disease, autoimmune disease or immune-mediated disease in a human. 37. A pharmaceutical composition according to any one of claims 1 to 33 or a pharmaceutical composition according to claim 34 or 35 for the prophylaxis and / or treatment of cancer, tumor, inflammatory disease, autoimmune disease or immune-mediated disease. 37. The method of claim 36 or 37 wherein said cancer is caused by an epithelial growth factor receptor (EGFR) tyrosine kinase or variant thereof, for the prevention and / or treatment of cancer, or for the prevention and / A pharmaceutical composition or pharmaceutical formulation. 39. The method of claim 38, wherein said cancer is caused by an EGFR tyrosine kinase or variant thereof, which involves EGFR exon 20 insertion or EGFR exon 19 deletion (Del19) or EGFR L858R mutation or EGFR T790M mutation, or any combination thereof.
A method for preventing and / or treating cancer or a pharmaceutical composition or pharmaceutical formulation for preventing and / or treating cancer. A pharmaceutical composition for the prophylaxis and / or treatment of cancer according to any one of claims 36, 38 and 39 or a method for the prevention and / or treatment of cancer according to any one of claims 37 to 39, A pharmaceutical dosage form for preventing and / or treating cancer according to any one of the preceding claims, wherein said cancer is lung cancer, preferably NSCLC, particularly NSCLC lung cancer, or a pharmaceutical composition or pharmaceutical composition Formulation. A dry granule for the manufacture of a pharmaceutical formulation comprising as active ingredient a compound of formula 1, or a pharmaceutically acceptable salt thereof, or a hydrate of a pharmaceutically acceptable salt thereof, and one or more excipients, Manufacturing method:
[Chemical Formula 1]

1.1 premixing one or more low melting point stabilizers, the pharmaceutically active ingredient, a portion of the at least one lubricant, the at least one binder and the at least one diluent;
1.2 Dry granulation of the premix of step 1.1 using a dry granulator to obtain granules;
2. Adding at least one disintegrant and at least one residual lubricant in one step or a subsequent step to the granules of step 1.2 and mixing to obtain a final blend;
3. compressing the final blend from the previous step into a tablet core using a tablet machine;
4.1 optionally suspending the ready-to-use coating mixture at room temperature with a mixture of purified water and alcohol to obtain a film-coated suspension; And
4.2 Optionally, coating the tablet cores obtained in step 3 with the film-coated suspension of step 4.1. A dry granule for the manufacture of a pharmaceutical formulation comprising as active ingredient a compound of formula 1: or a pharmaceutically acceptable salt thereof, or a hydrate of a pharmaceutically acceptable salt thereof, and at least one excipient, Manufacturing method:
[Chemical Formula 1]

1.1 pre-mixing PEG 8000, the pharmaceutically active ingredient, a portion of magnesium stearate, hydroxypropylcellulose, microcrystalline cellulose and mannitol;
1.2 Dry granulation of the premix of step 1.1 using a dry granulator to obtain granules;
2. Adding crospovidone and residual magnesium stearate to the granules obtained in step 1.2 in a step or in a subsequent step and mixing to obtain a final blend;
3. compressing the final blend of the previous step into a tablet core using a tablet machine;
4.1 optionally suspending the ready-to-use coating mixture at room temperature with a mixture of purified water and alcohol to obtain a film-coated suspension; And
4.2 Optionally, coating the tablet cores obtained in step 3 with the film-coated suspension of step 4.1. A pharmaceutical formulation obtainable according to the process of claim 40 or 41.

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